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Meis1和Pbx同源结构域蛋白家族的成员协同结合牛CYP17的一个cAMP反应序列(CRS1)。

Members of the meis1 and pbx homeodomain protein families cooperatively bind a cAMP-responsive sequence (CRS1) from bovine CYP17.

作者信息

Bischof L J, Kagawa N, Moskow J J, Takahashi Y, Iwamatsu A, Buchberg A M, Waterman M R

机构信息

Department of Biochemistry, Vanderbilt University School of Medicine, Nashville, Tennessee 37232-0146, USA.

出版信息

J Biol Chem. 1998 Apr 3;273(14):7941-8. doi: 10.1074/jbc.273.14.7941.

DOI:10.1074/jbc.273.14.7941
PMID:9525891
Abstract

The mammalian Pbx homeodomain proteins provide specificity and increased DNA binding affinity to other homeodomain proteins. A cAMP-responsive sequence (CRS1) from bovine CYP17 has previously been shown to be a binding site for Pbx1. A member of a second mammalian homeodomain family, Meis1, is now also demonstrated to be a CRS1-binding protein upon purification using CRS1 affinity chromatography. CRS1 binding complexes from Y1 adrenal cell nuclear extract contain both Pbx1 and Meis1. This is the first transcriptional regulatory element reported as a binding site for members of the Meis1 homeodomain family. Pbx1 and Meis1 bind cooperatively to CRS1, whereas neither protein can bind this element alone. Mutagenesis of the CRS1 element indicates a binding site for Meis1 adjacent to the Pbx site. All previously identified Pbx binding partners have Pbx interacting motifs that contain a tryptophan residue amino-terminal to the homeodomain that is required for cooperative binding to DNA with Pbx. Members of the Meis1 family contain one tryptophan residue amino-terminal to the homeodomain, but site-directed mutagenesis indicates that this residue is not required for cooperative CRS1 binding with Pbx. Thus, the Pbx-Meis1 interaction is unique among Pbx complexes. Meis1 also cooperatively binds CRS1 with the Pbx homologs extradenticle from Drosophila melanogaster and ceh-20 from Caenorhabditis elegans, indicating that this interaction is evolutionarily conserved. Thus, CYP17 CRS1 is a transcriptional regulatory element containing both Pbx and Meis1 binding sites, which permit these two homeodomain proteins to bind and potentially regulate cAMP-dependent transcription through this sequence.

摘要

哺乳动物的Pbx同源结构域蛋白可赋予其他同源结构域蛋白特异性,并增强其与DNA的结合亲和力。先前已证明牛CYP17的一个cAMP反应序列(CRS1)是Pbx1的结合位点。现在还证实,使用CRS1亲和层析纯化后,第二个哺乳动物同源结构域家族的成员Meis1也是一种CRS1结合蛋白。来自Y1肾上腺细胞核提取物的CRS1结合复合物同时包含Pbx1和Meis1。这是首个被报道为Meis1同源结构域家族成员结合位点的转录调控元件。Pbx1和Meis1协同结合CRS1,而这两种蛋白单独都无法结合该元件。CRS1元件的诱变表明Meis1的结合位点与Pbx位点相邻。所有先前鉴定的Pbx结合伙伴都具有Pbx相互作用基序,该基序在同源结构域的氨基末端含有一个色氨酸残基,这是与Pbx协同结合DNA所必需的。Meis1家族成员在同源结构域的氨基末端含有一个色氨酸残基,但定点诱变表明该残基并非与Pbx协同结合CRS1所必需的。因此,Pbx-Meis1相互作用在Pbx复合物中是独特的。Meis1还与果蝇的Pbx同源物extra denticle和秀丽隐杆线虫的ceh-20协同结合CRS1,这表明这种相互作用在进化上是保守的。因此,CYP17 CRS1是一个转录调控元件,包含Pbx和Meis1结合位点,这使得这两种同源结构域蛋白能够结合,并可能通过该序列调控cAMP依赖性转录。

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